medication safety and high alert medications - nebraska med · • high alert medications not...
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Medication Safety and High Alert Medications
Objectives
At the completion of this presentation participants should:
1. Be able to identify what a high alert medication is and what medications are considered high alert at Nebraska Medicine (NM)
2. Identify best practice recommendations and organizational safeguards used to reduce risk with high alert medications
3. Understand how to safely evaluate, order and monitor high risk medications
4. Understand the importance of medication warnings and the work being done to evaluate warnings to make existing warnings more meaningful
High Alert Medications
• High-alert medications are those medications that bear a heightened risk of causing significant patient harm when they are used in error
• Nebraska Medicine Pharmacy and Therapeutics Committee identifies medications that require safeguards at any step of the medication management process based on review of internal and external medication error and/or sentinel event data
• Several strategies and safeguards are instituted to ensure high alert medications are procured, stored, ordered, prepared, dispensed, and administered safely
High Alert Medications
• Strategies and safeguards implemented for high alert medications
• Use of “High Alert” stickers in applicable storage areas
• Use of red bins in applicable storage areas
• Labeling of applicable medications with a “High Alert” sticker when not already labeled as such by the manufacturer
• High alert medications not stored in a lock lidded pocket must be scanned when removed from the automated dispensing cabinet
• Whenever possible, ordering is restricted to order-sets
• When ordering a high alert medication the provider is required to select an appropriate indication
• Medications identified as high alert are labeled as such within One Chart
• Smart infusion pumps with guardrails are used
• Selected high alert medications require independent dual clinician verification prior to administration
High Alert Medications
• Per organizational policy MM02 High Alert Medications, the following medications and medication classes have been identified as being high alert at Nebraska Medicine
• Antithrombotics and specific anticoagulant agents
• Insulin
• Adrenergic agonists and inotropic agents
• Anesthetic and sedative agents
• Neuromuscular blocking agents
• Chemotherapy and other cytotoxic agents
• Concentrated electrolyte solutions
• Parenteral nutrition
• Prostacyclin analogues
• Epidural/intrathecal medications and patient controlled analgesia
• Sodium citrate/calcium infusions for CVVHD
• Nonformulary infusions
Antithrombotics & Anticoagulant Agents
• Includes abciximab, continuous infusion alteplase, argatroban, bivalirudin, intravenous unfractionated heparin (UFH), and eptifibitide
Safeguards that Impact Providers Yes No
Available concentrations are limited
Order-sets should be used when placing orders
Administration/monitoring instructions should be reviewed & defined by provider at the time of order entry
Required monitoring
Laboratory monitoring (ie. PTT or Hep Quant Assay, CBC)
Heparin
• UFH for continuous IV infusion should be ordered in a weight based fashion • Non weight-based dosing for small and pediatric patients is
dangerous!
• Pharmacokinetics is non-linear: a fixed dose of heparin will not predictably result in a fixed response
• Non-weight based heparin infusions are allowed for procedures related to thrombolysis IR or vascular patency.
• These infusions must be on a dedicated pump, and the pump must be appropriately labeled.
• Weight-based dosing of UFH for continuous infusion allows for uniform use of smart pump drug libraries
Heparin • UFH administered by continuous IV infusion requires
laboratory monitoring • Anti-Xa assay (heparin quantitative assay; HEPQT) is the
“gold standard”. A therapeutic aPTT is defined as one which correlates to a heparin quantitative assay of 0.3-0.7 IU/mL.
• Anti-Xa assay is less sensitive to some confounders that can affect aPTT (anti-phospholipid antibodies, DIC, congenital coagulation factor deficiency, etc.)
• Per the Pediatric Quality Committee only HEPQT can be used to monitor pediatric patients on heparin at NM
• Laboratory monitoring should also include:
• Baseline aPTT to confirm it is within normal range and rule out potential confounding conditions
• Platelet count prior to initiation and regularly to detect possible heparin-induced thrombocytopenia (HIT)
• Hemoglobin
Heparin • Heparin Protocol (CP RX_16)
• Developed to support a workflow that enhances safety and minimizes errors
• Applies to heparin infusions for Acute Coronary Syndrome/Cardiac, VTE/PE, Pediatrics, and Custom orders
• The pharmacist and nurse will collaborate to ensure appropriate dosing, adjustments and boluses are administered when ordered
Heparin
• When UFH is used per protocol, a provider must be contacted by a pharmacist or nurse in the following situations:
• When the patient weight is 177.8kg (VTE) or 181.9 kg (ACS) or greater at initiation
• Heparin quantitative assay results meet/exceed 1.1 units/mL, or the PTT results meet/exceed 200 seconds
• When the patient shows signs of active bleeding the nurse will contact the provider
• When infusing doses exceed the soft and/or hard maximum guardrail smart infusion device limit, the pharmacist will notify the provider. This is required for dose increases only
Heparin
• DVT/PE Treatment • Achieving therapeutic anticoagulation within 24 hours of
starting UFH improves outcomes (recurrent/progressive DVT/PE, death from PE, post-thrombotic syndrome) when treating DVT/PE1
• Use of an algorithm that uses weight based heparin dosing + standardized dose adjustments is more likely to achieve therapeutic anticoagulation in the first 24 hours2
• Exceptions might be necessary for patients with high bleeding risk (thrombocytopenia, additional anti-platelet agents, etc.)
1. Hull et al. Arch Intern Med 1992; 152: 1589 2. Raschke et al. Ann Intern Med 1993; 119: 874
Heparin
• Acute Coronary Syndrome (ACS) • Most patients receive additional agents that affect
coagulation system (anti-platelet agents, GPIIb/IIIa inhibitors, etc); therefore doses and therapeutic targets are generally lower than for PE/DVT
• Bleeding risks often higher because of concomitant anticoagulants
• Use of standard doses with nomograms for dose adjustments have not shown to directly affect outcome (survival, recurrent MI, bleeding), but most studies are preceding ‘modern’ interventions
• Because most studies using UFH are older, almost all studies used aPTT for monitoring and it is therefore not possible to firmly recommend a particular anti-Xa level for optimal therapy
Heparin • Custom UFH continuous infusion
• If the custom heparin protocol is used:
• The provider must order a discrete dose and indicate an appropriate therapeutic goal based off of Heparin Assay or aPTT. No custom algorithms will be allowed
• When a custom heparin infusion is ordered the provider must be contacted for each lab value outside of the ordered goal
Anticoagulant Exclusion Order • A “No anticoagulant or antiplatelet medications” order is available if a
provider determines that neither anticoagulant nor antiplatelet medications should be administered to a patient
• The exclusion order is similar to other medication orders, and once ordered will fire an alert to all end-users that attempt to order a medication that has been deemed inappropriate using the exclusion order
• Per policy (MS 66 Anticoagulation Management) the team indicated in the Service/Team responsible for order field should be contacted prior to making any changes to the exclusion order
Insulin
• Includes insulin formulations
Safeguards that Impact Providers Yes No
Available concentrations are limited
Order-sets should be used when placing orders
Administration/monitoring instructions should be reviewed & defined by provider at the time of order entry
Required monitoring
Hemoglobin A1C within past 90 days
Point of care glucose
1. Low prioritization of glycemic control in hospitalized patients
2. Medical status changes leading to alterations of insulin requirements
a. Release of counter-regulatory hormones
b. Decrease in insulin requirement
3. Variation of nutritional status
a. Changes in caloric intake
b. Transitions in the type of nutrition provided
4. Medication effects
a. Increased risk for HYPERglycemia
i. Calcineurins (e.g., tacrolimus, cyclosporine)
ii. Catecholamines
iii. Corticosteroids
b. Increased risk for HYPOglycemia
i. Insulin
ii. Quinolone antibiotics
iii. Tapering OR Withdrawal of corticosteroids
iv. Sulfonylureas
5. Knowledge deficits of healthcare providers
Barriers to Glycemic Control
• Insulin is the PRIMARY treatment option for diabetics while they are hospitalized
• Patients admitted to the hospital should have previous oral/non-insulin pharmacotherapy DISCONTINUED
• Institutional blood sugar goal for diabetic patients: 70 – 180 mg/dL
• Consider the BBCs of insulin therapy in ALL Type 1 and most Type 2 hospitalized diabetic patients:
Basal: long acting (insulin glargine) / intermediate acting (NPH)
Bolus [if eating]: rapid acting (insulin lispro)
Correction scale: rapid acting (insulin lispro)
Insulin Background
• BOTH over/under treatment of hyperglycemia create safety concerns when considering:
Changes in carbohydrate OR food intake
Changes in clinical status OR medications
Failure to adjust therapy based on blood
glucose (BG) patterns
Prolonged use of correction insulin
Poor coordination of BG testing with insulin
administration and meal delivery
Poor communication during patient transfers
Errors in placing orders
Hyperglycemia
Joint Commission Requirements Related to Diabetes Management
• Documentation of HbA1C:
MUST be drawn on ALL patients with diabetes if not current within the last 90-days
If available from an outside facility The result MUST be documented in the
electronic medical record (EMR)
If not drawn secondary to confounding results (e.g., recent blood transfusion)
The reason MUST be documented in the EMR
If the pre-checked box on the “General Subcutaneous Insulin” order set is UNCHECKED The reason MUST be documented in the
EMR
• Decide if the patient needs scheduled basal insulin
• When starting insulin in patients, utilize weight-based estimates
Dosing of Insulin
If the patient has these features present. . . Total Daily Dose (TDD) of insulin
(units/kg)
Malnourished, elderly (> 70 y.o.), CKD (on dialysis), severe liver disease
0.3
Normal-weight patients (including Type 1 diabetics) 0.4
Overweight 0.5
Obese, high dose steroids, or other markers of significant insulin resistance
0.6
Use a basal insulin in patients with known diabetes if. . .
Use a basal insulin in patients with or without a history of diabetes if. . .
• Type 1 diabetic OR otherwise markedly insulin deficient
• Patient already requires insulin • Poor control despite oral agents
• The patient consistently has a fasting blood glucose out of the target range
Dosing of Insulin Cont.
Nutritional Status
Necessary insulin components
Preferred regimen
NPO OR
Clear Liquids
Basal insulin: 50% of TDD Nutritional insulin: NONE
Basal insulin: glargine given once daily Nutritional insulin: NONE Correction: Rapid-acting/Regular insulin Q6H
Eating Meals
Basal insulin: 50% of TDD Nutritional Insulin: 50% of TDD divided equally before each meal
Basal insulin: glargine given once daily Nutritional insulin: rapid-acting analogue (RAA) insulin given with first bite of meal Correction: same RAA insulin as nutritional
Continuous Tube Feeds OR
Bolus Tube Feeds
Basal insulin: 40% of TDD Nutritional insulin: 60% of the TDD
Basal insulin: glargine given once daily Nutritional: RAA insulin Q4H OR regular insulin Q6H Correction: same insulin as nutritional
• The total daily dose (TDD) of insulin is the daily amount of insulin required for the patient
Encompasses both basal and nutritional needs of the patient
Order half of TDD as basal insulin given at the same time each day
Order the other half of TDD as rapid-acting insulin given in 3 equally divided doses (AC)
• Patients on previous outpatient insulin therapy
REDUCE insulin dose by 20 – 25% to prevent inpatient hypoglycemia
• Perioperative patients
Basal insulin should be REDUCED by at least 20%
Dosing of Insulin Cont.
Insulin Pharmacokinetics
Onset Peak Effect Duration of Action
Nutritional/Correction Insulin
Rapid-acting analog (aspart, glulisine, lispro*)
5 - 15 minutes 1 - 2 hours 4 - 6 hours
Regular* 30 - 60 minutes 2 - 3 hours 6 - 10 hours
Intermediate Insulin
NPH* 2 - 4 hours 4 - 10 hours 12 - 18 hours
Basal Insulin
Glargine* 2 - 4 hours Relatively “peakless”
20 - 24 hours
Detemir 2 hours Relatively “peakless”
16 - 24 hours
* = Preferred formulary agent
• Continuous infusion insulin should be transitioned to subcutaneous insulin therapy when the patient begins to eat and blood glucose levels are STABLE TIP: Guidance on how to transition a patient from
continuous infusion insulin to basal insulin can be found in the “General Subcutaneous Insulin” order-set
Transitioning from an Insulin Drip
• Subcutaneous BASAL insulin should be administered at least 1-2 hours PRIOR to discontinuing the infusion
• To ensure the insulin infusion is discontinued at the appropriate time
TIP: Utilize the inpatient consult to pharmacist order located in the “General Subcutaneous Insulin” order-set
• Order correction insulin based on the total daily dose
(TDD) of insulin needed by the patient
Level 1: < 40 units/day
Level 2: 40-80 units/day
Level 3: > 80 units/day
Transitioning from an Insulin Drip Cont.
Step 1: Establish the 24-hour insulin requirement by extrapolating from the
average IV insulin dose required over the previous 6-8 hours (if stable)
Example: Patient has been receiving 4 units/hr for the past 8 hours
– TDD of insulin = 3 units/hr X 8 hours X 3 = 72 units of insulin/day
Step 2: Take 60-80% of the extrapolated total daily insulin dose (TDD) calculated in step 1 above 72 units of insulin/day X 0.75 = 54 units of insulin/day
Give one-half as long-acting insulin preparation for basal coverage
72 units X 0.5 = 27 units of glargine daily
Give the other half as rapid-acting insulin divided by 3 for meal coverage doses
27 units of lispro ÷ 3 = 9 units of lispro AC
Step 3: Order correction insulin based upon the TDD of insulin needed
Level 1: < 40 units/day
Level 2: 40-80 units/day
Level 3: > 80 units/day
Example Transition from an Insulin Drip
• Patients receiving concurrent insulin therapy are at risk for hypoglycemia anytime therapy is interrupted
• Extended interruptions should be reviewed carefully to ensure an appropriate insulin regimen is ordered
Insulin Administration with Parenteral and Enteral Nutrition
Non-formulary Insulin Products
• NOT ALLOWED for the treatment of inpatients
• Pose a significant patient safety issue as outlined in “High Alert Medication Management” policy [MM02]
• Such products include: Toujeo
® (insulin glargine U-300)
Humalog® U-200 (insulin lispro)
Tresiba® (insulin degludec U-100, U-200)
Regular U-500
V-Go® insulin delivery devices
Insulin Pumps
• When an insulin pump is continued in the inpatient setting
FOLLOW the “Guidelines for Patient’s own Subcutaneous Insulin Pump” policy [MP 03 ] NM Campus: Endocrinology and Inpatient
Diabetes Education Services MUST be consulted
BMC Campus: The primary ordering provider is responsible for insulin pump orders OR an alternative insulin regime. Inpatient Diabetes Services are also available.
• The “Hyperkalemia Treatment (insulin)” order panel should ALWAYS be utilized
Insulin for the Treatment of Hyperkalemia
Adrenergic Agonists & Inotropic Agents
• Includes DOBUTamine, DOPamine, EPINEPHrine, Isoproterenol, Milrinone, Norepinephrine, Phenylephrine, Vasopressin
Safeguards that Impact Providers Yes No
Available concentrations are limited
Order-sets should be used when placing orders
Administration/monitoring instructions should be reviewed & defined by provider at the time of order entry
Required monitoring: Heart rate, blood pressure, SP02, and ECG monitoring
Adrenergic Agonists & Inotropic Agents
• When titration for a medication is necessary
• A range dose should always be used
• Administration instruction must provide guidance on how the nurse should titrate
Adrenergic Agonists & Inotropic Agents
• When a fixed dose for a medication is necessary
• A range dose should not be used
• Administration instructions should not contain titration information
Anesthetic & Sedative Agents
• Includes dexmedetomidine, etomidate, ketamine, methohexital, midazolam, propofol
• Must be ordered and administered in accordance with MS15 Sedation and Analgesia Administration Guidelines
Safeguards that Impact Providers Yes No
Available concentrations are limited
Order-sets should be used when placing orders
Administration/monitoring instructions should be reviewed & defined by provider at the time of order entry
Required monitoring
Heart rate, blood pressure, SP02, and ECG monitoring
Special monitoring for sedation (i.e. goal sedation score)
Anesthetic & Sedative Agents
• Special Monitoring for Sedation
• Titrations must be directed by an objective sedation or analgesic goal set by the provider
• Unless indicated by the provider:
• Sedation regimens will be titrated to a standard goal Richmond Agitation-Sedation Score (RASS) of -2 to 0
• Ordered analgesic regimens will be titrated to a standard goal pain score of Critical-Care Pain Observation Tool (CPOT) <3 or Behavioral Pain Scale (BPS) <5
• Patients must have spontaneous awakening trial daily, unless contraindicated/precluded by the awakening safety screen indicated in the ABCDE bundle
Neuromuscular Blocking Agents (NMB’s)
• Includes cisatricurium, rocuronium, succinylcholine, vecuronium
Safeguards that Impact Providers Yes No
Available concentrations are limited
Order-sets should be used when placing orders
Administration/monitoring instructions should be reviewed & defined by provider at the time of order entry
Required monitoring
Heart rate, blood pressure, SP02, and ECG monitoring
Special monitoring – When intended for prolonged use, an objective measurement of neuromuscular blockade must be used (i.e. train of four) and an objective measurement of sedation (i.e. BIS) must be used
Chemotherapy & Other Cytotoxic Agents
• Chemotherapy orders must be signed by an attending physician and verified by two pharmacists
Safeguards that Impact Providers Yes No
Available concentrations are limited
Order-sets, treatment plans, or therapy plans should be used when placing orders
Administration/monitoring instructions should be reviewed & defined by provider at the time of order entry
Required monitoring
Dependent on the chemotherapy regimen ordered
Chemotherapy & Other Cytotoxic Agents
• When placing orders using treatment or therapy plans, to prevent errors always consider the following:
• Review height, weight, & BSA, and update if needed
• When propagating orders ensure the dose is correct and that the order has not been discontinued
• If a patient is instructed to discontinue a specific therapy, always discontinue the order in the treatment plan. If this is not done, errors can occur when the patient is seen at a later date for a different reason
• Review labs and update treatment plans based on lab results
• Remove default lab parameters in treatment plans when they are inappropriate
Concentrated Electrolyte Solutions
• Includes calcium gluconate vials, magnesium sulfate vials, potassium chloride vials, calcium chloride vials, magnesium 40 g/500 mL, sodium chloride greater than 0.9% (hypertonic saline)
• Standardized orders for single electrolyte bolus doses will be available for selection during order entry
• Hypertonic saline
• Order sets are in development and will be utilized to enter hypertonic saline orders
• Pharmacists can order a serum sodium level 6 hours after administration of hypertonic saline to monitor for efficacy/toxicity
Parenteral Nutrition (PN)
• All PN orders expire 24 hours following initiation, and new orders must be placed each day
• A nutrition therapist must be consulted for all patients on PN
Safeguards that Impact Providers Yes No
Available concentrations are limited
Order-sets should be used when placing orders
Administration/monitoring instructions should be reviewed & defined by provider at the time of order entry
Required monitoring
Intake/Output recorded every 8 hours
Periodic assessment of electrolytes (BMP, Mg, Phos)
Point of care glucose testing should be considered
Prostacyclin Analogues • Includes intravenous epoprostenol and treprostinil
• A Pulmonary Medicine or Cardiology service must be consulted to manage therapy
• For initiation of therapy the patient must be admitted to an ICU as outlined in MS68 Levels of Care
• Patients that require hospitalization that are currently receiving chronic prostacyclin analogue therapy or are deemed stable following initiation may be admitted to the Adult Progressive Care Unit (APCU)
Safeguards that Impact Providers Yes No
Available concentrations are limited
Order-sets should be used when placing orders
Administration/monitoring instructions should be reviewed & defined by provider at the time of order entry
Required monitoring
Heart rate, blood pressure, respiratory rate, and SPO2 must be monitored with each dosing change
ECG monitoring
Epidural/Intrathecal Medications & Patient Controlled Analgesia (PCA)
• Only providers from Anesthesiology and Acute/Chronic Pain Service may administer epidural loading doses and bolus doses
• The provider must work with nursing staff to ensure the administration is documented in the MAR
Safeguards that Impact Providers Yes No
Available concentrations are limited
Order-sets should be used when placing orders
Administration/monitoring instructions should be reviewed & defined by provider at the time of order entry
Required monitoring
Continuous oximetry monitoring
Special monitoring identified within order-sets
Medication Administration
Medication Administration
• According to policy MS08 Administration of Parenteral Medications, licensed prescribers must have proficient knowledge of the following before administering a medication to a patient:
• Dose
• Administration technique
• Potential adverse effects
• Monitoring guidelines
Medication Administration
• Organization drug information resources (i.e. Lexicomp) are available on the Preceptor home page via the Drug Information link
Medication Administration
• Prior to administering a medication the following should be verified:
• The medication matches the order and product label
• There is no loss of medication integrity
• The medication is not expired
• No contraindications exist
• The correct medication is being administered at the proper time, in the prescribed dose, by the ordered route, and to the correct patient
• Barcode medication administration (BCMA) is used if available
• Unresolved concerns about the medication are discussed with the patient and/or appropriate providers
• The patient and/or family are informed of any potential significant adverse drug reactions or other concerns
One Chart Medication Warnings
One Chart Medication Warnings
• Alert end users of issues related to:
• Allergies
• Drug interactions
• Duplicate therapy
• Other potential medication issues
• Important for all individuals ordering medications to review medication warnings carefully
• For medication warnings to be effective, it is important to minimize alert fatigue by ensuring medication warnings are appropriate and meaningful
• Medication Safety Team and One Chart analyst run medication warning data every 3-6 months
• The following are reviewed quarterly by multiple groups and committees that include both pharmacists and physicians:
• Most common medication warnings
• Other opportunities related to warnings
• Special requests related to warnings
• Recommendations are reviewed and approved by the P&T Steering Committee prior to changes being made in One Chart
One Chart Medication Warnings